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首页> 外文期刊>The Biochemical Journal >Identification and characterization of a second 4,4 '-dibenzamido-2,2 '-stilbenedisulphonate (DBDS)-binding site on band 3 and its relationship with the anion/proton co-transport function
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Identification and characterization of a second 4,4 '-dibenzamido-2,2 '-stilbenedisulphonate (DBDS)-binding site on band 3 and its relationship with the anion/proton co-transport function

机译:谱带3上第二个4,4'-二苯甲酰氨基-2,2'-stilbenedisulphonate(DBDS)结合位点的鉴定和表征及其与阴离子/质子共转运功能的关系

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摘要

Band 3 mediates both electroneutral AE (anion exchange) and APCT (anion/proton co-transport). Protons activate APCT and inhibit AE with the same pK (similar to 5.0). SDs (stilbenedisulphonates) bind to a primary, high-affinity site on band 3 and inhibit both AE and APCT functions. In this study, we present fluorescence and kinetic evidence showing that lowering the pH activates a second site on band 3, which binds DBDS (4,4'-dibenzamido-2,2'-stilbenedisulphonate) independently of chloride concentration, and that DBDS binding to the second site inhibits the APCT function of band 3. Activation of the second site correlated with loss of chloride binding to the transport site, thus explaining the lack of competition. The kinetics of DBDS binding at the second site could be simulated by a slow-transition, two-state exclusive binding mechanism (R-0 <-> T-0 + D <-> TD <-> RD, where D represents DBDS, R-0 and T-0 represent alternate conformational states at the second DBDS-binding site, and TD and RD are the same two states with ligand DBDS bound), with a calculated overall K-d Of 3.9 mu M and a T-0 + D <-> TD dissociation constant of 55 nM. DBDS binding to the primary SD site inhibited approx. 94% of the proton transport at low pH (K-1 = 68.5 +/- 11.8 nM). DBDS binding to the second site inhibited approx. 68% of the proton transport (K-1 = 7.27 +/- 1.27 mu M) in a band 3 construct with all primary SD sites blocked through selective cross-linking by bis(sulphosuccinimidyl)suberate. DBDS inhibition of proton transport at the second site could be simulated quantitatively within the context of the slow-transition, two-state exclusive binding mechanism. We conclude that band 3 contains two DBDS-binding sites that can be occupied simultaneously at low pH. The binding kinetic and transport inhibition characteristics of DBDS interaction with the second site suggest that it may be located within a gated access channel leading to the transport site.
机译:带3介导电中性AE(阴离子交换)和APCT(阴离子/质子共转运)。质子以相同的pK(类似于5.0)激活APCT并抑制AE。 SD(二苯乙烯二磺酸盐)结合到频段3上的主要高亲和力位点,并抑制AE和APCT功能。在这项研究中,我们提供了荧光和动力学证据,表明降低pH值可激活条带3上的第二个位点,该位点独立于氯离子浓度结合DBDS(4,4'-二苯甲酰胺-2,2'-stilbenedisulphonate),并且DBDS结合第二位点的激活抑制了带3的APCT功能。第二位点的激活与氯离子与转运位点的结合丧失有关,因此解释了缺乏竞争。 DBDS在第二个位点的结合动力学可以通过缓慢过渡的两个状态的排他性结合机制来模拟(R-0 <-> T-0 + D <-> TD <-> RD,其中D代表DBDS, R-0和T-0代表第二个DBDS结合位点的交替构象状态,TD和RD是结合了配体DBDS的相同两个状态),计算出的总Kd为3.9μM,T-0 + D TD解离常数为55nM。 DBDS绑定到主要SD站点抑制约。在低pH值下(K-1 = 68.5 +/- 11.8 nM)质子传输的94%。 DBDS结合到第二个站点抑制约。带3构建体中68%的质子转运(K-1 = 7.27 +/- 1.27μM),所有主要SD位点均通过双(磺基琥珀酰亚胺基)硫酸盐的选择性交联而被阻断。 DBDS在第二个位置对质子运输的抑制作用可以在慢转变,两个状态的排他性结合机制的背景下进行定量模拟。我们得出的结论是,条带3包含两个DBDS结合位点,可以在低pH下同时被占据。 DBDS与第二个位点相互作用的结合动力学和运输抑制特性表明它可能位于通往运输位点的门控通道内。

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